Patologias do sistema urinário de cães e gatos / Diseases of the urinary tract of cats and dogs

Sapin, Carolina da Fonseca

19 February 2016

Submitted by Ubirajara Cruz (ubirajara.cruz@gmail.com) on 2017-06-26T15:49:03Z No. of bitstreams: 2 license_rdf: 0 bytes, checksum: d41d8cd98f00b204e9800998ecf8427e (MD5) Carolina_Sapin.pdf: 1243520 bytes, checksum: e9ae4587ba4ba0e8a1905c812da97edf (MD5) / Approved for entry into archive by Aline Batista (alinehb.ufpel@gmail.com) on 2017-06-27T19:05:07Z (GMT) No. of bitstreams: 2 Carolina_Sapin.pdf: 1243520 bytes, checksum: e9ae4587ba4ba0e8a1905c812da97edf (MD5) license_rdf: 0 bytes, checksum: d41d8cd98f00b204e9800998ecf8427e (MD5) / Made available in DSpace on 2017-06-27T19:05:07Z (GMT). No. of bitstreams: 2 Carolina_Sapin.pdf: 1243520 bytes, checksum: e9ae4587ba4ba0e8a1905c812da97edf (MD5) license_rdf: 0 bytes, checksum: d41d8cd98f00b204e9800998ecf8427e (MD5) Previous issue date: 2016-02-19 / Coordenação de Aperfeiçoamento de Pessoal de Nível Superior - CAPES / Nesta dissertação, abordam-se as patologias do sistema urinário. Os dados referentes a estas enfermidades são relacionados aos casos diagnosticados na região sul do Rio Grande do Sul em um período de 36 anos. Com base nesses achados foram elaborados dois artigos científicos. No primeiro trabalho avaliaram-se todas as lesões do sistema urinário de cães, constantes nos protocolos de necropsia e exames histopatológicos do Laboratório Regional de Diagnóstico da Faculdade de Veterinária da Universidade Federal de Pelotas, no período de 1978 a 2014. Foram encontrados diagnósticos de afecções do sistema estudado em 363 cães, correspondente a 4,04% do total de 8980 diagnósticos realizados no período para a espécie. As lesões renais representaram 93,1%, sendo 309 primárias do rim; dentre as principais lesões estavam a nefrite túbulo-intersticial (142 casos), geralmente associada à 47 casos de Leptospirose. O trato urinário inferior (TUI) representou 6,9% dos casos destacando-se a cistite aguda com 19 casos de um total de 60 lesões do TUI. Neste estudo a insuficiência renal, aguda ou crônica, representou importante causa mortis em cães. No segundo artigo descreve-se um diagnóstico anatomo-patológico de metaplasia disontogênica uretral em um felino fêmea, de um mês de idade e sem raça definida. Havia histórico de aumento de volume abdominal desde o nascimento. Ainda apresentava disúria, eliminando a urina apenas por cistocentese, sondagem vesical ou gotejamento. Foi eutanasiado e na necropsia observou-se bexiga aumentada e dilatada, rins diminuídos e ureteres dilatados e tortuosos. Histologicamente havia metaplasia disontogênica da uretra e displasia renal bilateral. Conclui-se nesta dissertação que as principais lesões renais foram a necrose tubular aguda, nefrite túbulo-intersticial, fibroplasia e glomeruloesclerose; e quanto ao TUI sobressaíram-se a cistite aguda, urolitíase, ruptura de bexiga e neoplasias primárias. / This thesis addresses the pathologies of the urinary system. The data concerning disorders of the urinary tract are related to cases diagnosed in southern Rio Grande do Sul in a period of 36 years. Based on these findings two papers were written. The first article assessed all the urinary tract lesions of canine, described in the necropsy reports and histopahtological tests from the Regional Laboratory of Diagnosis of the College of Veterinary in the Federal University of Pelotas in the period from 1978 to 2014. From a total of 8980 diagnosis, 363 dogs were found to have affections of the urinary system, which represents 4,04% of diagnosis performed for that period and species. Renal injury accounted for 93.1% of the cases, with 309 being primary kidney lesions; from which the main lesions were the tubulointerstitial nephritis (142 cases) often associated with Leptospirosis (47). Injuries of the lower urinary tract (LUT) accounted for 6.9% of the cases where acute cystitis stands out with 19 cases of a total of 60 LUT injuries. In this study, renal failure, acute or chronic, represented an important cause of death in dogs. The second article describes an anatomopathological diagnosis of dysontogenic urethral metaplasia in a female, one monthold, mongrel cat. The animal had history of abdominal enlargement since birth and dysuria, eliminating urine only cystocentesis, urinary catheterization or drip. It was euthanized and in the necropsy was observed enlarged and distended bladder, reduced kidneys and dilated and tortuous ureters. Histologically, it had dysontogenic metaplasia of the urethra and bilateral renal dysplasia. It is concluded in this thesis that the main renal lesions were acute tubular necrosis, tubulointerstitial nephritis, fibroplasia and glomerulosclerosis; and when the LUT is concerned, acute cystitis, urolithiasis, bladder rupture and primary neoplasms stood out.

Veterinária

Cão

Nefrite túbulo-intersticial

Trato urinário

Metaplasia disontogênica

Cistite aguda

Dog

Tubulointerstitial nephritis

Urinary tract

Dysontogenic metaplasia

Acute cystitis

Efeito antinociceptivo do HC-030031, um antagonista seletivo do receptor de potencial transitÃrio anquirina subtipo 1 (TRPA1), em modelos de nocicepÃÃo visceral. / Antinociceptive effect of HC-030031, a selective antagonist of transient receptor potential ankirin subtype 1 (TRPA1), on experimental models of visceral nociception.

Lus Mario da Silva Pereira

12 August 2012

A famÃlia de receptores de potencial transitÃrio (TRP) incluindo o receptor de potencial transitÃrio anquirina, subtipo 1 (TRPA1) tem mostrado ser um alvo terapÃutico potencial para o tratamento da dor aguda e crÃnica. Alguns estudos tÃm demonstrado que a resposta nociceptiva somÃtica se deve à ativaÃÃo dos receptores TRPA1 e sÃo efetivamente modulados atravÃs da ferramenta experimental, HC-030031, um antagonista seletivo. Contudo, existem poucos estudos que avaliam o papel dos receptores TRPA1 na dor visceral. Portanto, investigamos o papel do TRPA1 em modelos animais de nocicepÃÃo visceral induzido por diferentes substÃncias e tambÃm exploramos os possÃveis mecanismos envolvidos. Camundongos Swiss, machos (N=6) receberam carboximetilcelulose 0,5% (veÃculo CMC 0,5%, 1 mL/Kg, v.o.), HC-030031 (75, 150 ou 300 mg/Kg, v.o.), ou L-NAME (10 e 40 mg/Kg, s.c.) ou somente L-Arginina (600 mg/Kg, i.p.), 1 h apÃs foi administrado uma Ãnica injeÃÃo de IFO (400 mg/Kg, i.p.). A nocicepÃÃo visceral foi avaliada atravÃs do teste de Von Frey eletrÃnico previamente (T0) e 12 h (T1) apÃs a injeÃÃo de IFO com estimulaÃÃo abdominal atravÃs de um analgesÃmetro digital. Os resultados foram obtidos em gramas (T0-T1) pela variaÃÃo da hiperalgesia. Em seguida as bexigas dos animais foram removidas para pesagem, anÃlise e foram atribuÃdos escores macro e microscopicamente. Investigou-se, tambÃm, o efeito antinociceptivo visceral do HC-030031 atravÃs do modelo de nocicepÃÃo visceral induzido por Ãleo de mostarda (OM). Os animais foram tratados com CMC 0,5%, HC-030031 (18,75; 37,5 ou 75 mg/kg, v.o.) ou Morfina (5 mg/Kg, s.c.) isoladamente ou receberam Naloxona (2 mg/Kg, i.p.) previamente a estas drogas. Em seguida, OM 0,75% (50 &#956;L/colon) foi instilado localmente no cÃlon. A nocicepÃÃo visceral foi verificada atravÃs do teste de Von Frey previamente (T0) e 10 min. (T1) apÃs a injeÃÃo do OM. Em outro protocolo experimental, os animais foram tratados com CMC 0,5% (10 mL/kg, v.o.) ou HC-030031 (18,75; 37,5 ou 75 mg/Kg, v.o.) previamente a uma injeÃÃo intraperitoneal com Ãcido acÃtico 0,6% (AA, 10 mL/Kg,), zymosan (Zym, 1 mg/cavidade) ou misoprostol (MPT, 1 Âg/cavidade, um anÃlogo estÃvel de prostaglandinas). Imediatamente apÃs a injeÃÃo desses algogÃnicos, contabilizaram-se as contorÃÃes abdominais por 30 min. Adicionalmente, para investigar o papel de cÃlulas peritoneais residentes sobre o efeito do HC-030031, a cavidade peritoneal dos camundongos foi lavada com uma soluÃÃo de 30 mL (PBS + heparina) e os estÃmulos AA, Zym e MPT foram injetados i.p. Um grupo Sham foi incluÃdo tambÃm neste protocolo. Ao final do experimento, as contorÃÃes abominais foram registradas por 30 mim. Utilizou-se para a anÃlise estatÃstica, ANOVA/Student e Newman/Keul, foi considerado significativo um p < 0,05 (CEPA: Protocolo: 92/10). A IFO induziu significativa (p<0,05) nocicepÃÃo visceral (6,25Â1,08) e resposta inflamatÃria [escores edema 2(1-3); hemorragia 3(1-3) e peso bexiga (42,78 3,10)] comparado com o grupo salina (1,97Â0,89),[ 0(0-0); 0(0-0) e 20,01 0,7749] respectivamente. AlÃm disso, HC-030031(75 mg/Kg) e L-NAME (10 e 40 mg/Kg) preveniram de maneira significativa (p<0,05) da resposta nociceptiva (2,30Â1,07; 1,58Â0,86 e 0,2500  0,73) respectivamente quando comparado com o grupo IFO. O prÃ-tratamento com L-Arginina (6,844Â1,235) reverteu o efeito antinociceptivo do L-NAME 10 mg/Kg, (6,84Â1,23), mas foi ineficaz sobre o efeito do L-NAME 40 mg/Kg (1,500Â0,7361) e HC-030031 75 mg/Kg (0,7200Â0,6953). Contudo, o prÃ-tratamento com HC-030031 nÃo apresentou efeito antiinflamatÃrio. Adicionalmente, verificou-se que o OM induziu significativo (p<0,05) comportamento nociceptivo (6,333Â0,9458) quando comparado ao grupo salina (1,250Â0,9204). AlÃm disso, o HC-030031 preveniu de maneira significativa da resposta nociceptiva provocada pelo OM (1,536 Â0,7653). Avaliou-se tambÃm o envolvimento do sistema opiÃide no efeito antinociceptivo do HC-030031. Verificou-se que a morfina apresentou uma importante atividade antinociceptiva (0,07143Â0,07143) contra a nocicepÃÃo induzida por OM a qual foi significativamente revertida pelo prÃ-tratamento com naloxona (3,125 1,302). Por outro lado, o efeito antinociceptivo do HC-030031 nÃo foi afetado pela naloxona (2,240Â1,263). Adicionalmente, AA, Zym e MPT induziram respostas de contorÃÃes abdominais significativas (43,71Â4,43; 11,00Â2,11 e 9,00Â2.30, respectivamente) as quais foram significativamente inibidas com HC-030031 (18,75, 37,5 ou 75 mg/kg, v.o.) em todas as doses utilizadas no teste com AA (29,07%; 53,35% e 41,59%), no teste com Zym (55,85%; 61,03% e 71,20%) e no teste com MPT (63,88%; 83,33% e 88,88%). Uma vez que a prostaglandina ativa o nociceptor diretamente, demonstrou-se que o HC-030031 possivelmente inibe a nocicepÃÃo visceral atravÃs da estabilizaÃÃo direta de nociceptores. O efeito antinociceptivo do HC-030031 parece ser independente da inibiÃÃo de cÃlulas residentes inflamatÃrias, do Ãxido nÃtrico ou do sistema opiÃide. Este estudo fornece perspectivas para o manuseio da dor visceral atravÃs da modulaÃÃo dos canais TRPA1. / The description of the TRP family of receptors including TRPA1 has provided potential therapeutic targets for treating acute and chronic pain. Some studies have shown a somatic nociceptive response due to the TRPA1 receptors activation which is effectively modulated with the experimental tool, HC-030031, a TRPA1 antagonist. However, there are a few studies evaluating the role of TRPA1 receptors in visceral pain. Then aimed to investigate the role of TRPA1 in the animal models of visceral nociception induced by different substances and to explore the possible mechanisms involved. Swiss male mice (n=6) were given only Carboxymethyl cellulose (vehicle CMC 0.5%, 1 mL/kg, p.o.), the compound HC-030031 (75, 150 or 300 mg/Kg, p.o.) or L-NAME (10 or 40 mg/Kg, s.c.) alone or with L-arginine (600mg/Kg, i.p.) 1h previously a alone injection of IFO (400 mg/kg, i.p.). Visceral nociception was assessed through the von Frey test previously (T0) and 12h (T1) later IFO injection by the abdominal stimulation with a pressure meter. The results were obtained in grams (T0-T1). The bladder of these animals were also removed to weighted (BWW), analyzed and after given scores macro and microscopically. We also investigated the antinociceptive effect of HC-030031 in the model of mustard oil-induced visceral nociception. The animals were treated with CMC 0.5% or HC-030031 (18.75, 37,5 or 75 mg/kg) or Morphine (5 mg/Kg, s.c.) alone or with Naloxone (2 mg/Kg, i.p.) 1h previously the injection of Mustard oil (MO) 0,75% (MO, 50 ul/colon). Visceral nociception was assessed through the von Frey test previously (T0) and 10 min (T1) after MO injection by the abdominal stimulation with a pressure meter. The results were obtained in grams (T0-T1). In another experimental setting, the animals were treated with CMC 0.5% (1 mL/kg, p.o) or HC-030031 (18.75; 37.5 or 75mg/Kg, p.o.) previously an intraperitoneal injection with acetic acid 0.6% (AA, 10 mL/kg), zymosan (Zym, 1 mg/cavity) or misoprostol (MPT, a stable prostaglandin analogous, 1&#956;g/cavity) and immediately had the writhing responses counted for 30 min. In order to investigate the role of resident peritoneal cells on the effect of HC-030031, we washed the peritoneal cavity of mice with heparin added PBS (30 mL) and then AA, Zym or MPT were injected i.p. A Sham group was included. Eventually, the writhing responses were recorded. Statistical analysis was performed with ANOVA/Student Newman Keul as appropriate. p<0.05 was accepted. (CEPA: Protocol 92/10). IFO induced significant (p<0.05) visceral nociception (6.25Â1.08) and inflammatory response [scores to edema 2(1-3); hemorrhage 3(1-3); and bladder wet weight (42.78  3.1)] in comparison with saline treated group (1.97Â0.89), [0(0-0); 0(0-0); 20.01 0.7749] respectively. Moreover, HC-030031(75) and L-NAME (10 or 40 mg/Kg) prevented in a significant manner (p<0.05) the nociceptive response (2.30Â1.07; 1.58Â0.860 and 2500Â0.7361) respectively when compared with IFO-treated group. Although the pretreatment with L-arginine (6.844Â1.235) was able to reverse the antinoceceptive effect of L-NAME 10 mg/Kg, (6.84Â1.23), it failed to do the same (p>0.05) with L-NAME 40 mg/Kg (1.500Â0.7361) and HC-0300031 75 mg/Kg (0.72Â0.69). The same reversible effect of L-Arginine was observed for the anti-inflammatory activity of L-NAME (p<0.05). However, HC-030031 presented no anti-inflammatory effect. The antinociceptive activity of HC-030031 was also assessed in the MO nociception model. We verified that MO induced a significant (p<0.05) nociceptive behavior (6.333Â0.9458) when compared to saline injected mice (1.250Â0.9204). Moreover, HC-030031 prevented in a significant manner the nociceptive response elicited by MO (1.536Â0.7653). Furthermore, the involvement of opioid system in the antinociceptive effect of HC-030031 as tested. We observed that morphine presented an important antinociceptive activity (0.07143Â0.07143) against MO-induced nociception which was significantly reverted by naloxone pre-treatment (3.125 1.302). On the other hand, the antinociceptive effect of HC-030031 remained in spite the injection of naloxone (2.240Â1.263). In addition to that, AA, Zym and MPT induced significant writhing responses (43.71Â4.43; 11.00Â2.11; 9.00Â2.30; respectively) which was significantly inhibited with HC-030031(18.75, 37.5 e 75 mg/kg, p.o.) treated mice in all the doses tested (29.07%, 53.35% and 41.59%, in the AA test, 55.85%, 61.03% and 71.20%, in the Zym test, 63.88%, 83.33% and 88.88%, in the MPT induced nociception, respectively to 18.75, 37.5 and 75 mg/kg doses. Eventually, the reduction of cell population in the peritoneal cavity prevented the development of writhing responses in both AA and Zym injected mice, with no effect was visualized on MPT treated mice. We the conclude that, since prostaglandin activates the nociceptor directly, it was shown that HC-030031 inhibits visceral nociception possibly through the stabilization of the neuronal ends. The antinociceptive effect of HC-030031 seems to be independent of the inhibition of inflammatory resident cells, opioid and nitric oxide pathways. This study provides perspective for the effective management of visceral pain through the modulation of TRPA1 channels.

NocicepÃÃo Visceral

Cistite HemorrÃgica

HC-030031

visceral nociception

hemorrhagic cystitis

HC-030031

FARMACOLOGIA

The 2017 Update of the German Clinical Guideline on Epidemiology, Diagnostics, Therapy, Prevention, and Management of Uncomplicated Urinary Tract Infections in Adult Patients. Part II: Therapy and Prevention

Kranz, Jennifer, Schmidt, Stefanie, Lebert, Cordula, Schneidewind, Laila, Mandraka, Falitsa, Kunze, Mirjam, Helbig, Sina, Vahlensieck, Winfried, Naber, Kurt, Schmiemann, Guido, Wagenlehner, Florian M.

26 May 2020

Background: We aimed to update the 2010 evidence- and consensus-based national clinical guideline on the diagnosis and management of uncomplicated urinary tract infections (UTIs) in adult patients. Results are published in 2 parts. Part 1 covers methods, the definition of patient groups, and diagnostics. This second publication focuses on treatment of acute episodes of cystitis and pyelonephritis as well as on prophylaxis of recurrent UTIs. Materials and Methods: An interdisciplinary group consisting of 17 representatives of 12 medical societies and a patient representative was formed. Systematic literature searches were conducted in MEDLINE, EMBASE, and the Cochrane Library to identify literature published in 2010–2015. Results: For the treatment of acute uncomplicated cystitis (AUC), fosfomycin-trometamol, nitrofurantoin, nitroxoline, pivmecillinam, and trimethoprim (depending on the local rate of resistance) are all equally recommended. Cotrimoxazole, fluoroquinolones, and cephalosporins are not recommended as antibiotics of first choice, for concern of an unfavorable impact on the microbiome. Mild to moderate uncomplicated pyelonephritis should be treated with oral cefpodoxime, ceftibuten, ciprofloxacin, or levofloxacin. For AUC with mild to moderate symptoms, instead of antibiotics symptomatic treatment alone may be considered depending on patient preference after discussing adverse events and outcomes. Primarily non-antibiotic options are recommended for prophylaxis of recurrent urinary tract infection. Conclusion: In accordance with the global antibiotic stewardship initiative and considering new insights in scientific research, we updated our German clinical UTI guideline to promote a responsible antibiotic use and to give clear hands-on recommendations for the diagnosis and management of UTIs in adults in Germany for healthcare providers and patients.

info:eu-repo/classification/ddc/610

ddc:610

Biomarkers in the Light of the Etiopathology of IC/BPS

Neuhaus, Jochen, Berndt-Paetz, Mandy, Gonsior, Andreas

04 May 2023

In this review, we focused on putatively interesting biomarkers of interstitial cystitis/bladder pain syndrome (IC/BPS) in relation to the etiopathology of this disease. Since its etiopathology is still under discussion, the development of novel biomarkers is critical for the correct classification of the patients in order to open personalized treatment options, on the one hand, and to separate true IC/BPS from the numerous confusable diseases with comparable symptom spectra on the other hand. There is growing evidence supporting the notion that the classical or Hunner-type IC (HIC) and the non-Hunner-type IC (NHIC) are different diseases with different etiopathologies and different pathophysiology at the full-blown state. While genetic alterations indicate close relationship to allergic and autoimmune diseases, at present, the genetic origin of IC/BPS could be identified. Disturbed angiogenesis and impairment of the microvessels could be linked to altered humoral signaling cascades leading to enhanced VEGF levels which in turn could enhance leucocyte and mast cell invasion. Recurrent or chronic urinary tract infection has been speculated to promote IC/BPS. New findings show that occult virus infections occurred in most IC/BPS patients and that the urinary microbiome was altered, supporting the hypothesis of infections as major players in IC/BPS. Environmental and nutritional factors may also influence IC/BPS, at least at a late state (e.g., cigarette smoking can enhance IC/BPS symptoms). The damage of the urothelial barrier could possibly be the result of many different causality chains and mark the final state of IC/BPS, the causes of this development having been introduced years ago. We conclude that the etiopathology of IC/BPS is complex, involving regulatory mechanisms at various levels. However, using novel molecular biologic techniques promise more sophisticated analysis of this pathophysiological network, resulting in a constantly improvement of our understanding of IC/BPS and related diseases.

info:eu-repo/classification/ddc/610

ddc:610

CCL2 (MCP-1) MEDIATES CHRONIC PELVIC PAIN THROUGH MAST CELLS IN EXPERIMENTAL AUTOIMMUNE CYSTITIS

Bicer, Fuat

28 August 2012

No description available.

Biochemistry

Biology

Health Sciences

Medicine

Molecular Biology

Neurosciences

CCL2

MCP-1

Chronic Pelvic Pain

Mast Cell

Experimental Autoimmune Cystitis

IC PBS

Uroplakin 3A

Bladder

Efeitos colaterais tardios na bexiga após radioterapia por câncer de colo de útero: avaliação da associação com polimorfismos de TP53, ATM e MDM2 / Late urinary bladder side effects after radiotherapy for cervical cancer: evaluation of the association with TP53, ATM and MDM2 polymorphisms

Pinezi, Juliana Castro Dourado

13 October 2014

Introdução: Na prática clínica se observa que há diferenças na incidência de efeitos colaterais entre pacientes submetidos ao mesmo esquema terapêutico de radioterapia. Tais diferenças podem ser entendidas como uma radiossensibilidade individual determinada geneticamente. Objetivos: Este estudo teve como objetivo avaliar os efeitos tardios na bexiga em pacientes com câncer do colo uterino tratadas com radioterapia, com ou sem cirurgia, e o valor prognóstico de três polimorfismos genéticos de base única com relação ao desenvolvimento de cistite actínica. Material e métodos: Foi realizada uma análise retrospectiva de 50 pacientes com carcinoma cervical tratadas entre 1999 e 2004, com um mínimo de 6,5 anos de seguimento. A dose de radioterapia na bexiga foi considerada como a soma da dose da radioterapia externa com a dose de braquiterapia no ponto de bexiga definido pelo ICRU 38 (Relato número 38 da Comissão Internacional de Unidades e Medidas em Radiação). Para as correlações entre dose e efeito, foi calculada a dose biológica efetiva (BED) para cada caso. Para a avaliação dos efeitos tardios em bexiga, além dos dados descritos em prontuário, foi feito um questionário específico dirigido aos sintomas urinários, foi realizada cistoscopia em todas as pacientes e a escala LENTSOMA (efeitos tardios no tecido normal/ subjetivo-objetivo tratamento e exames) foi aplicada, utilizando o pior grau do efeito encontrado nos diferentes métodos de avaliação. Variantes genéticas do códon 72 da p53 (Arginina / Prolina), MDM2 SNP309 T/G e ATMex39 5557 G>A foram identificadas usando o método de genotipagem de SNP ABI SNaPshot e os resultados foram correlacionados com a incidência e grau de cistite actínica. Resultados: Complicações clínicas tardias da bexiga foram registradas em 17 (34%) pacientes usando dados coletados dos prontuários e em 41 (82%) pacientes pelo questionário de existência e gravidade dos efeitos tardios da irradiação. Essas complicações foram diretamente correlacionadas com a BED. Vinte e oito pacientes (56%) desenvolveram cistite diagnosticada por cistoscopia (16% Grau 2-4). MDM2 SNP309 TT associado a TP53 (P72R) GG foram relacionados com o aumento da incidência de cistite. Conclusões: Cistite actínica, em grau 2 ou maior, foi elevada nessa população e apresentou uma maior incidência quando realizado um questionário específico para tal. Houve associação com maior dose de radioterapia (BED Gy3 > 100 Gy) e com MDM2 SNP309 TT associado a TP53 (P72R) GG. / Introduction: In clinical practice it is observed that there are differences in the incidence of side effects among patients undergoing the same regimen of radiotherapy. Such differences can be understood as a genetically determined individual radiosensitivity. Purposes: This study aimed to evaluate urinary bladder late effects in patients with uterine cervix cancer treated with radiotherapy with or without surgery and the prognostic value of three single nucleotide polymorphisms (SNPs) related to radiation cystitis. Material and methods: retrospective analysis of 50 patients with cervical carcinoma treated between 1999 and 2004 with a minimum of 6.5 years of follow-up was performed. The radiation dose in the bladder was considered as the dose delivered by external beam irradiation plus the brachytherapy dose in the ICRU Report 38 (International Commission of Radiation Units and Measurements report number 38) bladder point. For dose-effect correlations the biological effective dose (BED) was calculated for each case. For evaluation of bladder late effects, besides the data collected from the charts review, a specific query directed to urinary symptoms was applied to the patients and also a cystoscopy was performed in all of them. The LENTSOMA (late effects of normal tissues/subjective-objective management analytic) scale for bladder late effects was applied. Genetic variants of p53 codon72 (arginine/proline) polymorphism, MDM2 SNP309 T/G and ATMex39 5557G>A were identified by using ABI SNaPshot SNP genotyping method. And the results were correlated with the incidence and grade of radiation cystitis. Results: Clinical late bladder complications were recorded in 17 (34%) patients using data collected from the charts and in 41 (82%) patients by the questionnaire for the existence and severity of late irradiation effects. These complications were directly related with the BED. Twenty eight patients (56%) developed cystitis diagnosed by cystoscopy (16% Grade 2-4). MDM2 SNP309 TT associated with TP53 (P72R) GG was related with increased incidence of cystitis. Conclusions: Late radiation cystitis grade 2 or greater were high in this population and presented a higher incidence when a specific questionnaire was used. Higher radiation dose (BED Gy3 > 100 Gy) and MDM2 SNP309 TT associated with TP53 (P72R) GG were correlated with bladder late effects

Brachiterapy

Braquiterapia

Cistite

Cystitis

Genes p53

Genes p53

Ionizing radiation

Neoplasias do colo do útero

Proteins muteins ataxia telangiectada

Proteins ubiquitins ligases

Radiação ionizante

Radioterapia

Radiotherapy

Ubiquina-proteína ligases

Uterine cervical neoplasms

Avaliação clínico-laboratorial da obstrução uretral em felinos domésticos

Schaefer, Gabriela da Cruz

January 2017

A obstrução uretral é uma condição clínica comum em gatos, caracterizada por alterações metabólicas e do equilíbrio hidroeletrolítico e ácido-básico que são potencialmente fatais. Dentre as causas de obstrução uretral, a cistite idiopática é a mais frequentemente observada em diversos estudos. Outras causas incluem urolitíase, tampões uretrais e infecção do trato urinário. Em muitos casos, os gatos encontram-se em estado crítico e a morte pode ocorrer em decorrência de alterações metabólicas, como estado urêmico avançado e hipercalemia. As principais alterações eletrolíticas e do equilíbrio ácido-básico relatadas são hipercalemia, acidose metabólica, hiponatremia e hipocalcemia ionizada. Embora a obstrução uretral seja muito frequente na rotina clínica, estudos para caracterizar a população de gatos acometida ainda são escassos no Brasil. Características relacionadas ao manejo, dieta e perfil dos tutores podem influenciar na manifestação da doença. Os objetivos do presente estudo foram avaliar os parâmetros clínicos e as alterações hematológicas, bioquímicas, urinárias, eletrolíticas e ácido-básicas presentes em gatos com obstrução uretral e a associação entre estas variáveis. Além disso, objetivou-se conhecer as principais causas de obstrução uretral nos gatos atendidos no Hospital de Clínicas Veterinárias da Universidade Federal do Rio Grande do Sul. Para isso, foram incluídos no estudo 28 gatos com diagnóstico de obstrução uretral no período de dezembro de 2015 a dezembro de 2016. Foram obtidos dados referentes ao histórico, exame físico, coletados sangue e urina, além da realização de exames de imagem (radiografia e ultrassonografia abdominal). Em todos os gatos foram realizados hemograma, bioquímica sérica, análise de pH, gases e eletrólitos sanguíneos, urinálise e urocultura. Após, todos os pacientes foram tratados de acordo com um protocolo pré-estabelecido. A causa mais comum de obstrução uretral neste estudo foi a cistite idiopática, que ocorreu em mais de 60% dos casos, seguida de tampões uretrais e infecção do trato urinário. Nenhum caso de urolitíase foi diagnosticado, o que pode ser explicado por fatores como idade, ambiente e estilo de vida dos animais. A maioria dos gatos obstruídos apresentou múltiplos sinais sistêmicos, assim como alterações metabólicas, eletrolíticas e do equilíbrio ácido-básico, principalmente azotemia, hiperlactatemia, acidose metabólica, hipercalemia e hipocalcemia ionizada. Hipotermia, depressão do estado mental, bradicardia e desidratação foram os parâmetros clínicos que tiveram maior quantidade de associação com as alterações metabólicas e podem ser considerados bons preditores clínicos destas desordens. Por outro lado, o lactato não foi considerado um bom preditor de alterações clínicas e laboratoriais neste estudo. / Urethral obstruction is a common and potentially life-threatening condition, characterized by severe metabolic, electrolyte and acid-base disturbances. Among the causes of urethral obstruction, idiopathic cystitis is the most frequent in several studies. Other causes include urolithiasis, urethral plugs and urinary tract infection. In many cases, cats are critically ill and death may occur due to metabolic alterations, such as advanced uremic status and hyperkalemia. The main electrolyte and acid-base balance disorders reported are hyperkalemia, metabolic acidosis, hyponatremia and ionized hypocalcemia. Although urethral obstruction is a very common condition, there are few studies characterizing the population affected by the disease in Brazil. Characteristics related to management, diet and owner’s profile can influence the manifestation of the disease. The aim of the present study was to evaluate the association of clinical, haematological, biochemical, urinary, hydroelectrolyte and acid-base parameters in male cats with urethral obstruction. In addition, the objective was to determine the causes of urethral obstruction in male cats admitted to the Veterinary Teaching Hospital of Federal University of Rio Grande do Sul. Twenty-eight cats diagnosed with urethral obstruction were included in the study between December 2015 and December 2016. Data regarding medical history and physical examination were obtained. Blood and urine were collected, and imaging tests were performed (abdominal radiography and ultrasonography). Complete blood count, serum chemistry, blood pH, gas and electrolyte, urinalysis and urine culture were performed. All patients were treated accordingly to a previous established protocol. The most common cause of urethral obstruction in this study was idiopathic cystitis, which occurred in more than 60% of cases, followed by urethral plugs and urinary tract infection. No diagnosis of urolithiasis was achieved which could be explained by factors like age, environment and life style of cats. Most of obstructed cats presented with multiple systemic clinical signs, as well as, metabolic, electrolyte and acid-base alterations. The main disorders found were azotemia, hyperlactatemia, metabolic acidosis, hyperkalemia and ionized hypocalcemia. Hypothermia, depressed mental status, bradycardia and dehydration were the clinical parameters with the greatest amount of associations with the metabolic alterations and can be considered as good predictors of metabolic disorders. On the other hand, lactate was not considered a good predictor of clinical and laboratory abnormalities in this study.

Trato urinario : Patologia

Cistite idiopática : Felinos

Desequilíbrio ácido-básico

Hipercalemia

Acidose metabólica

Obstrucao uretral

Clinica veterinaria : Felinos

Feline lower urinary tract disease

Idiopathic cystitis

Acid-base disorders

Hyperkalemia

Metabolic acidosis

Análise de polimorfismos de nucleotídeo único na cistite intersticial / Single nucleotide polymorphism analysis in interstitial cystitis

Cassão, Valter Dell Acqua

08 December 2017

IINTRODUÇÃO: A Cistite Intersticial (CI) ou Síndrome da Bexiga Dolorosa (SBD) é uma síndrome crônica caracterizada pela presença de dor ou desconforto vesical ou pélvico e sintomas miccionais como urgência e aumento da frequência miccional diurna e noturna, na ausência de outra afecção identificável que justifique esses sintomas. Não existe até o momento nenhum teste diagnóstico ou marcador que defina a CI. Desta forma seu diagnóstico é predominantemente clínico, baseado nos sinais e sintomas e dependente da exclusão de outras doenças urológicas. A dificuldade no diagnóstico e no tratamento dessas pacientes reflete o pouco que se sabe sobre sua fisiopatologia e sobre as alterações genéticas presentes na doença. A identificação de marcadores pode proporcionar um melhor entendimento e manejo desses aspectos da síndrome. Na tentativa de identificar marcadores genéticos que possam estar associados a CI, avaliamos a presença de alguns polimorfismos genéticos, os polimorfismos de nucleotídeo único (SNP), no DNA de pacientes com os critérios diagnósticos de CI e comparamos sua prevalência entre as pacientes e também com um grupo controle representativo da população geral. A correlação desses polimorfismos considerando a CI e a intensidade de dor nessas pacientes ainda não foi estudada na literatura. OBJETIVOS: Analisar a presença de polimorfismos (SNP) em amostras de sangue de pacientes com CI e correlacionar a presença dos polimorfismos com o quadro de dor crônica. MÉTODOS: Foram selecionadas 34 pacientes do sexo feminino com diagnóstico de CI de acordo com os critérios do NIDDK e 23 pacientes do grupo controle (mulheres saudáveis apenas com incontinência urinária de esforço). As pacientes com o diagnóstico de CI foram estratificadas em dois grupos de acordo com o grau dos sintomas de dor crônica. Foram selecionados 20 polimorfismos para análise: rs1800871, rs1800872, rs1800896, rs1800471, rs1800629, rs361525, rs1800497, rs6311, rs6277, rs6276, rs6313, rs2835859, rs11127292, rs2243248, rs6887695, rs3212227, rs1799971, rs12579350, rs3813034, rs6746030. A genotipagem foi realizada através da técnica de PCR em tempo real (q-PCR) e correlacionada com o diagnóstico de CI e com a intensidade dos sintomas álgicos. RESULTADOS: O alelo polimórfico (T) do SNP rs11127292 foi mais frequente nas pacientes com CI em relação ao grupo controle (p:0,01). O alelo polimórfico (T) do SNP rs6311 foi significativamente mais frequente nas pacientes com dor mais intensa (p:0,03). A frequência do alelo selvagem (A) do SNP rs1799971 foi maior em pacientes com dor leve a moderada (p:0,04). CONCLUSÕES: Foram identificadas algumas diferenças na frequência dos polimorfismos nas pacientes estudadas, o que sugere a existência de um papel relevante dos SNP associados tanto à CI quando na intensidade dos sintomas de dor crônica nestas pacientes / INTRODUCTION: Interstitial cystitis (IC) or painful bladder syndrome (PBS) is a chronic syndrome characterized by the presence of bladder/pelvic pain or discomfort and voiding symptoms such as urgency and increased urinary waking and night-time frequency in the absence of another identifiable cause to justify these symptoms. So far, there is no diagnostic test or marker to establish the presence of IC. Thus, the diagnosis is predominantly clinical, based on signs and symptoms and dependent on the exclusion of other urological diseases. The difficulty in the diagnosis and treatment of these patients reflects the little that is known about IC physiopathology and about the genetic background of the disease. The identification of new markers may provide a better understanding and management of the syndrome. As an attempt to identify genetic markers that may be associated with IC, we evaluated the presence of some genetic polymorphisms, single nucleotide polymorphisms (SNPs), in the DNA of patients with the diagnostic criteria of IC, and we compared their prevalence among IC patients and with a control group representative of the general population. The correlation of these polymorphisms considering IC and pain intensity in these patients has not been studied in the literature. OBJECTIVES: To assess the presence of polymorphisms (SNPs) in blood samples from IC patients and to correlate the presence of polymorphisms with chronic pain. METHODS: Thirty-four female patients with a diagnosis of IC according to the NIDDK criteria and 23 control subjects (healthy women with stress urinary incontinence) were selected. Patients with the diagnosis of IC were stratified into two groups according to the degree of symptoms of chronic pain. We selected 20 polymorphisms for analysis: rs1800871, rs1800876, rs1800471, rs1800629, rs361525, rs1800497, rs6311, rs6277, rs6276, rs6313, rs2835859, rs11127292, rs2243248, rs6887695, rs3212227, rs1799971, rs12579350, rs3813034, rs6746030. Genotyping was performed using the real-time PCR technique (q-PCR) and correlated with the diagnosis of IC and intensity of pain symptoms. RESULTS: The polymorphic allele (T) of the SNP rs11127292 occurred with more frequency in patients with IC compared to the control group (p= 0.01). The polymorphic allele (T) of SNP rs6311 occurred with more frequency in patients with severe pain (p= 0.03). The frequency of wild-type (A) SNP rs1799971 was higher in patients with mild to moderate pain (p= 0.04). CONCLUSION: The results indicated differences in polymorphism frequency in the patients studied, suggesting the existence of a relevant role of SNPs associated with both IC and intensity of chronic pain symptoms in these patients

Ache

Bladder pain syndrome

Cistite intersticial

Dor

Inflamação

Inflammation

Interstitial cystitis

Painful bladder syndrome

Polimorfismo

Polimorfismo de nucleotídeo único

Polymorphism

Síndrome de bexiga dolorosa

Síndrome de dor na bexiga

Single nucleotide polymorphism

Serum Amyloid A Protein (SAA) in Healthy and Infected Individuals

Lannergård, Anders

January 2005

<p>Serum amyloid A protein (SAA) is an acute phase protein that has recently gained increasing interest as a potential marker for disease and treatment monitoring. We investigated SAA and CRP levels in (a) patients with various common infectious diseases (n=98), (b) patients with pyelonephritis (n=37) versus patients with cystitis (n=32), (c) healthy individuals of varying ages (n=231), (d) very immature newborn infants with or without nosocomial infections (NIs) (n=72) and (e) patients with bacterial infections treated with cefuroxime (n=81). </p><p>SAA significantly correlated with CRP in viral as well as in bacterial infections (for the total group: r²=0.757, p<0.0001) and showed a systemic inflammatory response in 90% of the patients with cystitis as compared with 23% for CRP. Equally high efficiencies (0.96 and 0.94 for SAA and CRP, respectively) were observed in discriminating between pyelonephritis and cystitis. SAA and high sensitive (hs) CRP were lower in umbilical cords (p<0.0001) and higher in elderly adults (p<0.0001-0.03) than in the other age groups; higher in immature newborn infants than in term infants; and higher in the NI group than in the non-NI group. Interindividual variabilities of the time course of the biomarkers SAA and CRP were considerable. Because of the smoothed distribution of SAA and CRP (i.e. elevations were both essentially unchanged during the first 3 days of cefuroxime treatment), these markers were not useful when deciding parenteral-oral switch of therapy, which occurred within this time period in most cases.</p><p>SAA is a sensitive systemic marker in cystitis. SAA and hsCRP in umbilical cord blood are close to the detection limit and increase with age. They increase in relation to NI in very immature newborn infants and might therefore be used in diagnosis and monitoring. Finally, SAA and CRP in adults with bacterial infections could not predict an early parenteral-oral switch of antimicrobial therapy.</p>

Communicable diseases

acute phase proteins

adult

Administration Oral

aminoglycosides

amyloidosis

antibiotics

bacterial infections

body temperature

C-reactive protein

cefuroxime

cystitis

cytokines

elderly

infant

interleukin-6

newborn

pyelonephritis

serum amyloid A protein

virus diseases

Infektionssjukdomar

Infectious diseases

Infektionssjukdomar

Serum Amyloid A Protein (SAA) in Healthy and Infected Individuals

Lannergård, Anders

January 2005

Serum amyloid A protein (SAA) is an acute phase protein that has recently gained increasing interest as a potential marker for disease and treatment monitoring. We investigated SAA and CRP levels in (a) patients with various common infectious diseases (n=98), (b) patients with pyelonephritis (n=37) versus patients with cystitis (n=32), (c) healthy individuals of varying ages (n=231), (d) very immature newborn infants with or without nosocomial infections (NIs) (n=72) and (e) patients with bacterial infections treated with cefuroxime (n=81). SAA significantly correlated with CRP in viral as well as in bacterial infections (for the total group: r2=0.757, p&lt;0.0001) and showed a systemic inflammatory response in 90% of the patients with cystitis as compared with 23% for CRP. Equally high efficiencies (0.96 and 0.94 for SAA and CRP, respectively) were observed in discriminating between pyelonephritis and cystitis. SAA and high sensitive (hs) CRP were lower in umbilical cords (p&lt;0.0001) and higher in elderly adults (p&lt;0.0001-0.03) than in the other age groups; higher in immature newborn infants than in term infants; and higher in the NI group than in the non-NI group. Interindividual variabilities of the time course of the biomarkers SAA and CRP were considerable. Because of the smoothed distribution of SAA and CRP (i.e. elevations were both essentially unchanged during the first 3 days of cefuroxime treatment), these markers were not useful when deciding parenteral-oral switch of therapy, which occurred within this time period in most cases. SAA is a sensitive systemic marker in cystitis. SAA and hsCRP in umbilical cord blood are close to the detection limit and increase with age. They increase in relation to NI in very immature newborn infants and might therefore be used in diagnosis and monitoring. Finally, SAA and CRP in adults with bacterial infections could not predict an early parenteral-oral switch of antimicrobial therapy.

Communicable diseases

acute phase proteins

adult

Administration Oral

aminoglycosides

amyloidosis

antibiotics

bacterial infections

body temperature

C-reactive protein

cefuroxime

cystitis

cytokines

elderly

infant

interleukin-6

newborn

pyelonephritis

serum amyloid A protein

virus diseases

Infektionssjukdomar

Infectious diseases

Infektionssjukdomar